Deregulated calcium signaling in blood cancer: Underlying mechanisms and therapeutic potential

Tracey Immanuel; Jixia Li; Taryn N Green; Anna Bogdanova; Maggie L Kalev-Zylinska

doi:10.3389/fonc.2022.1010506

Deregulated calcium signaling in blood cancer: Underlying mechanisms and therapeutic potential

Front Oncol. 2022 Oct 18:12:1010506. doi: 10.3389/fonc.2022.1010506. eCollection 2022.

Authors

Tracey Immanuel¹, Jixia Li^{1

2}, Taryn N Green¹, Anna Bogdanova^{3

4}, Maggie L Kalev-Zylinska^{1

5}

Affiliations

¹ Blood and Cancer Biology Laboratory, Department of Molecular Medicine and Pathology, University of Auckland, Auckland, New Zealand.
² Department of Laboratory Medicine, School of Medicine, Foshan University, Foshan City, China.
³ Red Blood Cell Research Group, Institute of Veterinary Physiology, Vetsuisse Faculty, University of Zurich, Zürich, Switzerland.
⁴ Zurich Center for Integrative Human Physiology, University of Zurich, Zürich, Switzerland.
⁵ Haematology Laboratory, Department of Pathology and Laboratory Medicine, Auckland City Hospital, Auckland, New Zealand.

Abstract

Intracellular calcium signaling regulates diverse physiological and pathological processes. In solid tumors, changes to calcium channels and effectors via mutations or changes in expression affect all cancer hallmarks. Such changes often disrupt transport of calcium ions (Ca²⁺) in the endoplasmic reticulum (ER) or mitochondria, impacting apoptosis. Evidence rapidly accumulates that this is similar in blood cancer. Principles of intracellular Ca²⁺ signaling are outlined in the introduction. We describe different Ca²⁺-toolkit components and summarize the unique relationship between extracellular Ca²⁺ in the endosteal niche and hematopoietic stem cells. The foundational data on Ca²⁺ homeostasis in red blood cells is discussed, with the demonstration of changes in red blood cell disorders. This leads to the role of Ca²⁺ in neoplastic erythropoiesis. Then we expand onto the neoplastic impact of deregulated plasma membrane Ca²⁺ channels, ER Ca²⁺ channels, Ca²⁺ pumps and exchangers, as well as Ca²⁺ sensor and effector proteins across all types of hematologic neoplasms. This includes an overview of genetic variants in the Ca²⁺-toolkit encoding genes in lymphoid and myeloid cancers as recorded in publically available cancer databases. The data we compiled demonstrate that multiple Ca²⁺ homeostatic mechanisms and Ca²⁺ responsive pathways are altered in hematologic cancers. Some of these alterations may have genetic basis but this requires further investigation. Most changes in the Ca²⁺-toolkit do not appear to define/associate with specific disease entities but may influence disease grade, prognosis, treatment response, and certain complications. Further elucidation of the underlying mechanisms may lead to novel treatments, with the aim to tailor drugs to different patterns of deregulation. To our knowledge this is the first review of its type in the published literature. We hope that the evidence we compiled increases awareness of the calcium signaling deregulation in hematologic neoplasms and triggers more clinical studies to help advance this field.

Keywords: Calcium signaling; blood cells; calcium homeostasis; cancer biological pathways; leukaemia; lymphoma; myeloproliferative neoplasms; red cell abnormalities.

Publication types

Review